The search resulted in 6,209 potential articles from PubMed (n = 1,777), Cochrane Library (n = 95), Embase (n = 3,672), and Web of Science (n = 665). In total, 6,139 articles were excluded based on the double-blind screening of the title and abstract, including 904 duplicates. The remaining 70 full text articles were assessed, and 27 articles were found eligible for this review (21 RCT and 6 non-RCT).
Flow diagram.
Risk of bias assessment of randomized controlled trials.
Quality assessment according to the MINORS assessment tool.
Thyroxine in the “Block-and-Replace” regimen.
| Study | Country | Design | Sample | Sex(M:F) | Age(yrs) | Medication | Intervention process | Follow-up | Assessments | Results | Side effect | |
|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Bromberg et al. ( |
Brazil | RCT | 45 | A(4:28)/B(2:12) | A(range 17–55 years)/B(range 21–49 years) | A (40–100mg MMI or 400–900mg PTU+75ug T3)/B(5–25mg MMI or 50–300mg PTU) | duration of therapy was similar for both groups: range 12–26 months for group A, range 10–28 months for group B | before. during treatment and 5–6 weeks after withdrawal of ATD | T3, T4, TSH, FT4, TgAb, eye signs | no obvious difference in the improvement of Graves’ ophthalmopathy between the two treatment options | – | |
| Perozim et al. ( |
Brazil | Non-RCT | 28 | 4:24 | 14–53 | 40mg MMI + 75ug T4 | 60mg MMI (4–6 weeks) → 40mg MMI+ 75ug T4 (18–24 months) | 18–24 months MMI+L-T4 → additional 2 years after treatment | ultrasonographic, TBG, TRAb, T3, T4 | decreases TRAb and the frequency of recurrence of hyperthyroidism | – | |
| Edmonds and Tellez ( |
UK | RCT | 70 | HD(6:28)/TD(11:25) | HD(48 ± 11.9)/TD(41 ± 12.9) | HD (60mg Carb. +100–150mg T4)/TD (60mg Carb. → maintenance dose Carb.) | HD (4 weeks Carb. →1 year Carb. +T4), TD (4 weeks Carb. →1 year maintenance dose Carb.) | 2 years after stopping treatment (monthly→ 3-month intervals) | FT3, TSH, TRAb, TBG, pertechnetate uptakes, ophthalmopathy | measured variables and progress of patients was similar in the HD or TD regimen | HD (8), TD (6) | |
| Jorde et al. ( |
Norway | RCT | 56 | HD(5:24)/LD(6:21) | HD(40.6 ± 2.1)/LD(43.8 ± 2.8) | HD (60mg MMI+0.1–0.15mg T4)/LD (30mg MMI) | HD (2–4 weeks 60mg MMI→MMI+0.1–0.15mg T4), LD (30mg MMI→ dose titrated every 2–4 weeks), all treatment stop after 6 months | every 3 months (first 1 year) →every 6 months (the 2 year) | thyroid volume, T3, T4, TSH, eye symptoms | significantly reduced the relapse rate the 1 year, the relapse rates in both groups were unacceptably high | HD (9), LD (4) | |
| McIver et al. ( |
UK | RCT | 111 | A(11:41)/B(11:48) | A(33 ± 9)/B(36 ± 10) | A(maintenance dose Carb.)/B (40mg Carb. + 100ug T4) | 40mg Carb. (1 month)→group A (Carb. alone 17 months), group B (17 months Carb. +T4→T4 alone 18 months) | median follow-up period was 12 months | T3, T4, TSH, TRAb | neither delays nor prevents the recurrence of hyperthyroidism | 5(urticaria, arthralgia, nausea) | |
| Lucas et al. ( |
Spain | RCT | 60 | A(7:23)/B(4:26) | A(37.5 ± 13.9)/B(34.5 ± 8.3) | A(maintenance dose Carb.)/B(30–45mg Carb.+75–150ug L-T4) | 45–60 mg Carb.→divided into 2 groups, all treatment during 12–24 months | 3-month interval (first 2 years)→annually thereafter, or when relapse | T3, T4, FT4, TSH, TBG, goiter size, ophthalmopathy | offers no advantages in the treatment of GD | – | |
| Grebe et al. ( |
New Zealand | RCT | 37 | H(5:12)/L(3:17) | H(33 ± 8.7)/L(33.7 ± 11.9) | HD (100mg Carb. +T4)/LD (25mg→titrating dose Carb.) | all treatment discontinue after 6 months | every 6 weeks (first 3 months) → 3-monthly (first year) →6-monthly (the 2 year) | FT4, FT3, TSH, IgA, IgG, IgM, WBC, RBC | delays, but not prevent relapse | HD(7), LD(1) | |
| Nedrebo et al. ( |
Norway | RCT | 218 | 1A(0.148:0.152)/1B(0.161:0.839)/2A(0.074:0.926)/2B(0.166:0.834) | 1A(43.9 ± 10.2)/1B(40.2 ± 11.5)/2A(42.4 ± 12.2)/2B(43.4 ± 13.3) | 1A(Carb.+L-T4→L-T4)/1B (Carb.+L-T4→ no drugs)/2A (Carb.→L-T4)/2B(Carb.→ no drugs) | Carb. (12 months): group 1 (B&R therapy) and group 2 (titration regimen) →divided into 2 subgroups (1 year) | before treatment→ after 3 and 6 weeks→ every 3 months | TRAb, TSH, FT4, T3, size of goiter | relapse rates were independent of Carb. regimen whether followed by L-T4 therapy or not | rash (21) | |
| Vaidya et al. ( |
UK | Non-RCT | 450 | B&R(20.2:79.8)/Titration(13.4:86.6)/Both(17.9:82.1) | B&R(49 ± 15)/Titration(49 ± 18)/Both(48 ± 15) | B&R/Titration/Both titration and B&R | retrospectively examined case-records of patients with GD | when relapses (only included the first episode), treated more than 2 years (included the first 2 years) | FT4, FT3, TSH, TRAb, TPOAb | little evidence that patients under B&R have more stable thyroid function | skin rash (1.3%:6%), neutropenia (1.3%:0.7%), liver dysfunction (0%:0.7%) | |
Thyroxine addition in the titration regimen.
| Study | Country | Design | Sample | Sex(M:F) | Age(yrs) | Medication | Intervention process | Follow-up | Assessments | Results | Side effect |
|---|---|---|---|---|---|---|---|---|---|---|---|
| Hashizume et al. ( |
Japan | RCT | 109 | A1(7:22)/A2(6:21)/B1(7:24)/B2(4:18) | A1(36 ± 6)/A2(32 ± 7)/B1(33 ± 7)/B2(34 ± 6) | A1(100μg T4 +10mg MMI)/A2(placebo+10mg MMI)/B1 (same as A1)/B2(same as A2) | 30mg MMI (6 months) →divided into Group A (antibody level 15% or more) or B (antibody level less than 15%) → divided into 2 subgroups | stop MMI within 1 year after MMI+T4 therapy → T4 or placebo alone for 3 years | T3, T4, TSH, TBG, TRAb | decreases production of TRAb and relapse rate | not found |
| Kuo et al. ( |
China | Non-RCT | 60 | A(6:19)/B(5:10)/C(4:16) | A(34 ± 5)/B(37 ± 6)/C(36 ± 6) | A (10mg MMI +0.1mg T4)/B (10mg MMI)/C (10mg MMI) | 30mg MMI (3 months) →15mg MMI (3 months) →divided into 3 groups (6 months) | 6 months and 12 months of combination therapy | FT4, TSH, TRAb, TBG, T3, T4, thyroid volume | patients treated with MMI+T4 have greater decline in TRAb and TBG | – |
| Tamai et al. ( |
Japan | RCT | 105 | A(8:27)/B(9:26)/C(8:27) | A(35.3 ± 2.4)/B(36.8 ± 2.3)/C(36.2 ± 2.3) | A((maintenance MMI+75–100ug T4, TSH normal))/B(same as A, TSH suppressed)/C((maintenance dose MMI) | MMI (1 year)→divided into 2 groups→group 1:MMI+ T4/group 2: MMI (6 months) →group 1 divided into group A and B, group 2 as groupC(6 months) | 12 months after treatment | TSH, T4, FT4, FT3, TBG, TRAb | no effect on TRAb and rates of recurrence | – |
| Pfeilschifter and Ziegler ( |
Germany | RCT | 50 | A(2:8)/B(3:9)/C(7:21) | A(36.0 ± 15.1)/B(39.6 ± 13.3)/C(41.1 ± 10.2) | A (10mg Carb.+ low dose T4)/B(10mg Carb.)/C(10mg Carb.+ 50–150ug T4→T4) | 3 groups for 12 months treatment→ ATD discontinued after 1 year→suppressive doses T4 continued another year | 3-month intervals | TSH, T3, T4, TBG | unable to detect a preventive effect on the recurrence of hyperthyroidism, benefit for thyroid enlargement | not found |
| Rittmaster et al. ( |
Canada | RCT | 149 | 1(15:85)/2(14:86)/3(10:90) | 1(38 ± 14)/2(39 ± 14)/3(38 ± 13) | 1(30mg MMI →maintenance dose MMI)/2(30mg MMI→30mg MMI+ T4→T4)/3(30mg MMII→30mg MMI+T4→T4) | divided into 3 groups for 18 months: group 1(maintenance dose MMI)/group 2(MMI+T4) to maintain TSH 2.0–5.4mIU/L/group 3(MMI+T4) to maintain TSH ≤0.6mIU/L→T4 continue in group 2 and group 3(TSH in low-normal range or below normal) | 3–4 week intervals(first 6 months) →every 2 months(6–18 months) →after methimazole stop 2 or 3 weeks to identify whether remission →if remission, every 1–2 months(next 2 yrs) → every 6–12 months | FT4, FT3, TSH, TRAb, thyroid size | addition of T4 to MMI does not improve long-term remission rates | rash and/or itching(41), joint or muscle discomfort(31), metallic taste(45), gastrointestinal complaints(9), jaw pain(2), agranulocytosis(1), hepatitis(2) |
| Raber et al. ( |
Austria | RCT | 114 | 1(11:89)/2(16:84)/3(18:82) | 1(40 ± 13)/2(41 ± 11)/3(43 ± 13) | group 1(MMI→ stop MMI)/group 2(MMI→10mg MMI+50ug- variable dose T3)/group 3(MMI→50ug- variable dose T3) | 60mg MMI for 1 week →40mg MMI for 1 week→20mg for week 3→adjust MMI on thyroid function (8.5 ± 7.4 weeks) → maintenance dose MMI (9.0 ± 2.5 months) →divided into 3 groups for 6 months: group 1(stop MMI)/group 2(MMI+T3) to suppress TSH <0.1mU/L/group 3(T3) to suppress TSH <0.1mU/L | every 3 weeks after diagnosis→ every 4–6 weeks throughout the study after divided into 3 groups (mean follow-up of 16 months) | T3, T4, FT4, TSH, TRAb, thyroid size, 24h urinary iodine excretion | no significant difference was seen in relapse | Palpitations (7), light-headedness (1), diarrhea (1), weight instability (1) |
| Glinoer et al. ( |
Belgium | RCT | 82 | 12.15:70.85 | mean age of 36 years | A (30–80mg ATD →25mg ATD+L-T4→L-T4)/B (30–80mg ATD → 25mg ATD+L-T4→no drugs) | Phase I: 30–80mg ATD (1 month) → 25mg ATD+85ug L-T4(4 month) → 25mg ATD+100ug L-T4(6 month) → 25mg ATD+110ug L-T4(9 month) → 25mg ATD+115ug L-T4(15 month) Phase II: randomly assigned into 2 group, A (100ug L-T4 for 12 months)/B (placebo) | Phase I: 1 (optional), 2, 4, 6, 9, 12, 15 months Phase II: every 3 months | FT4, FT3, TSH, TRAb | L-T4 administration during and after ATD withdrawal did not improve remission rate | – |
| Wu et al. ( |
China | RCT | 60 | A(4:16)/B(5:15)/C(5:15) | A(35 ± 7)/B(39 ± 6)/C(35 ± 5) | A(5–10mg MMI +50ug L-T4→50ug L-T4)/B(5–10mg MMI→5mg MMI)/C(5–10mg MMI +50ug L-T4→5mg MMI+50ug L-T4) | 30mg- maintenance dose MMI (6 months) → distributed into 3 groups (24 months) → A (6 months L-T4 alone), B (6 months MMI), C(6 months MMI+L-T4) | every 3 months within 1 year of discontinuation | FT3, FT4, TSH, TSAb | cannot reduce the recurrence rate more effectively than with only MMI | – |
| Hoermann et al. ( |
Germany | RCT | 225 | A(13:98)/B(16:98) | A(41 ± 1.87)/B(41 ± 1.10) | A(no drugs)/B(maintenance dose L-T4) | ATD (12–15 months) →divide into 2 groups for 1 year (4 weeks after drug withdrawal) →treatment based on test results (1 year) | 1, 3, 6, 12, 18, 24 months | FT3, FT4, TSH, T3, T4, TRAb, thyroid volume | not prevent relapse of hyperthyroidism after restoration of euthyroid function by ATD | – |
| Mastorakos et al. ( |
Greece | RCT | 108 | T4(6:27)/T3(8:30)/placebo (8:29) | T4(43.8 ± 11.6)/T3(42.6 ± 15.2)/placebo(43.1 ± 13.8) | T4(100μgT4)/T3(25μg T3)/placebo | ATD (24 months), assignment into 3 groups during the period | evaluated trimonthly up to 12 months and at 24 months. | TT3, TT4, FT3, FT4, TSH, TRAb, TPOAb, TgAb, thyroid weight, exopthalmos | T4 administration after ATD treatment is associated with increased recurrence compared to T3 or placebo | – |
| Liu et al. ( |
China | RCT | 145 | Group 1(7:39)/Group 2(6:41)/Group 3(9:43) | Group 1 (33.1 ± 10.9)/Group 2 (33.1 ± 12.3)/Group 3 (34.3 ± 13.9) | Group 1(30mg →5mg MMI)/Group 2 (30mg →15mg MMI→ 10mg MMI +L-T4→ 5mg+L-T4)/Group 3(30mg →10mg MMI→ 10mg+L-T4→ 5mg+L-T4→ 2.5mg+L-T4) | 30mg MMI (at least 1 month) → treat in 3 groups for 5 months (MMI, 30mg→20mg→15mg→10mg→5mg, add L-T4 when appropriate) | 1, 3, 6, 9, 12, 18, 24, 36, 48, 60 and 72 months after drug withdrawal | FT4, FT3, TSH, thyroid size | addition of L-T4 to MMI neither improves nor prevents the remission or recurrence | – |
| Yang et al. ( |
China | RCT | 109 | C(16:38)/I(17:38) | C(64.49 ± 3.39)/T(63.87 ± 3.16) | C(15–30 mg MMI → maintenance dose MMI)/T(15–30mg MMI +25ug L-T4→ maintenance dose MMI+25ug L-T4) | both groups treat for 18 months | after completion of treatment | TSH, FT3, FT4, TRAb, ALP, CT, 24h UP, 24h UCa, PTH, blood calcium, serum phosphorus, BMD | beneficial effect on bone metabolism in older patients, no difference in remission rates | – |
Thyroxine addition in special populations.
| Study | Country | Design | Sample | Sex(M:F) | Age(yrs) | Medication | Intervention process | Follow-up | Assessments | Results | Side effect | |
|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Hashizume et al. ( |
Japan | RCT | 78 | pregnancy | A (25.8 ± 4.1)/B (26.2 ± 4.2) | A (100ug T4)/B (no drugs) | euthyroid 2 months before pregnancy (10–30mg MMI for 1–3yr)→MMI discontinued 5–6 months after onset of pregnancy →divide into 2 groups:A (T4 continue for 1yr after delivery)/B(no drug) | 5–6 months after onset of pregnancy until 1 year after delivery | T3, T4, TBG, TSH, TRAb | decreases TRAb and prevent the postpartum recurrence | – | |
| Vigone et al. ( |
Italy | Non-RCT | 28 | 4:24 | average age is 9.2 years (ranging from 2.58 to 16.83 years) | MMI (average 0.3mg/kg/day) + L-T4 (average dose of 1.12μg/kg/day) | ATD (1.5 years) → poor control of thyroid function→ combination therapy for 2.85 years (ranging from 5 months to 7 years) | 2–4 weeks (first 6 months) →2–4 months, in case of remission (2–4 months in first 2 years→6–12 months) | ultrasonography, TSH, FT3, FT4, TT3, TT4 | better control of thyroid function, delay radioiodine treatment for 4.9 years and surgery for 2.9 years, not increase remission rates | neutropenia (1) | |
Non-pharmacological research of Graves’ disease.
| Study | Country | Design | Sample | Sex(M:F) | Age(yrs) | Medication | Intervention process | Follow-up | Assessments | Results | Side effect |
|---|---|---|---|---|---|---|---|---|---|---|---|
| Kaur et al. ( |
UK | RCT | 34 | Group 1(3:9)/group 2 (3:7)/group3 (3:9) | Group 1 (38y11 m ±8y1m)/group 2(34 y8 m ± 10y10 m)/group 3(32y 11m ±8y) | Group 1 (I2 alone)/group 2 (ATD+T4)/group 3((ATD+ T4+I2) | use ATD for 4–6 weeks until euthyroid →add L-T4 0.15–0.2mg. for 2–3 months →divide into 3 groups for 10 days preoperatively | 1 day preoperatively → the day after→ 5 days after operation | size of goiter, T4, FT4, vascularity of gland, operative blood loss, thyroid follicular size | addition of iodine preoperatively is unnecessary in the patient who is euthyroid on ATD and L-T4 | – |
| Tallstedt et al. ( |
Sweden | Non-RCT | 492 | A(20:80)/B(14:86) | A(60 ± 13)/B(59 ± 12) | A (maintenance dose T4)/B (0.05mg→0.1mg T4) | 131I therapy →group A received T4 (when hypothyroidism), group B received 0.05mg of T4(2 weeks after 131I) and 0.1mg (after further 2 weeks) | 18 months after therapy | size of thyroid, T3, T4, TSH, soft-tissue involvement, Optic nerve damage | early administration of T4 after 131I reduces the occurrence of Graves’ ophthalmopathy | – |
| Zhu et al. ( |
China | Non-RCT | 168 | C(82)/I(A23/B 21/C 25/D 17) | C(-)/I(-) | Control (MMI or PTU)/A (MMI or PTU)/B(same as A)/C(MMI or PTU)/D(same as C) | 45–90mg MMI or 45mg–900mg PTU→1.6pg/kg L-T4 or 40–60mg thyroid pills while continuing ATD (A/C is 2 months, B/D is 1 months) | 1 month (first 3 months) →every 3 months(1 year) | FT4, FT3, TSH, symptom rating Scale, thyroid crisis, injury to RLN, low calcium, bleeding | sequential thyroid defunctionalization followed by thyroxine supplementation reduce the bleeding volume and postoperative complication rate | – |
| Taïeb et al. ( |
European | RCT | 94 | group A(12:34)/group B(11:37) | group A (48.8 ± 13.5)/group B (47.1 ± 12.9) | group A(early prophylactic L-T4 treatment)/group B (L-T4 when needed) | group A(50µg L-T4, 5 days post-radioiodine→ dose adapted at 1, 3 and 6 months), group B(followed up every 4 weeks and treated with LT4 when needed) | 1, 3, 6,12 months post-RAI | FT4, FT3, TSH, TRAb, ThyPRO, QoL | Early LT4 administration post- RAI represent potential benefit for QoL. RAI activities and LT4 treatment dosage and timing remains to be determined | not reported |
ALP, alkaline phosphatase; ATD, antithyroid drugs; Carb., carbimazole; FT3, serum free triiodothyronine; FT4, free thyroxine; GD, graves’ disease; HD, high dose; HR, heart rate; HRQL, hypothyroid-health related quality of life; IL-6, interleukin-6; IL-8, interleukin-8; IL-10, interleukin-10; IgA, immunoglobulin A; IgG, immunoglobulin G; IgM, immunoglobulin M; LD, low dose; L-T4, levo-thyroxine; MAP, mean artery pressure; MMI, methimazole; PTH, parathyroid hormone; QoL, quality of life; RBC, red blood cells; RLN, recurrent laryngeal nerve; SBP, systolic blood pressure; T3, triiodothyronine; T4, thyroxine; TBG, thyroxine binding globulin; TgAb, thyroglobulin antibody; ThyPRO, thyroid specific patient-reported outcome; TPOAb, thyroid peroxidase antibody; TRAb, thyrotropin receptor antibodies; TSAb, thyroid stimulating antibody; TSH, thyroid stimulating hormone; TSQ, thyroid specific questionnaire; Uca, urine calcium; UP, urine phosphorus; WBC, white blood cell.
The “block-and-replace” (B&R) regimen is well known to endocrinologists, but it is not routinely recommended in clinical practice. The B&R regimen completely blocks the thyroid hormone synthesis with high-dose ATD, while supplementing exogenous thyroxine to replace normal thyroid function. As per the 2016 American Thyroid Association guidelines, B&R therapy should be avoided or, if necessary, should be used after addressing compliance, in patients whose condition was inadequately controlled with one dose of methimazole (MMI) and who then become hypothyroid after a minimal dose increase (
Three studies including Perozim et al., Jorde et al., and Grebe et al. reported that the B&R regimen had some benefits in the recurrence of Graves’ disease (
In four other clinical studies, including Edmonds and Tellez, McIver et al., Lucas et al., and Nedrebo et al., the results showed that the B&R regimen for the recurrence rate of Graves’ disease was not superior to titration therapy (
Therefore, the included studies showed that thyroxine addition during the B&R regimen or after stopping the ATD did not show more benefits than the titration regimen in the long-term recurrence rate of Graves’ disease.
The titration regimen is widely used in clinical practice. Throughout the course of the treatment, the dose of ATD is adjusted according to the condition and thyroid hormone concentrations, which can generally be divided into initial, decrement, and maintenance phases. There were 11 RCTs (
Among the 11 studies, only the study by Hashizume et al. showed a positive effect (
These results have not been confirmed in subsequent studies, and all the remaining nine studies drew contrary conclusions. Similar to the study by Hashizume et al. (
The treatment of Graves’ disease in special groups, such as children and pregnant women, has its special features. In the study by Hashizume et al., 78 patients with Graves’ disease received MMI for 1–3 years before pregnancy and thyroid function remained normal during the first two months of pregnancy (
Parents generally consider non-pharmacological treatments for children with Graves’ disease because of the poor compliance or severe side effects caused by ATD. Due to concerns about post-intervention complications, non-pharmacological treatments are often not accepted by children’s parents when the patient is very young (
Although such studies are few and insufficient as clinical evidence, they can also provide some basis for clinical treatment and further research.
Four of the clinical studies screened were on the non-pharmacological treatment of Graves’ disease, two of which were RCT (
Taïeb et al. randomly divided 94 patients with Graves
Kaur et al. randomly assigned 34 patients with Graves
From these results, some clinical benefits could be seen, but these studies were small in size and scattered in purpose. If these conclusions are to be confirmed, high-quality clinical research is needed.